Discovery of a Spontaneous Genetic Mouse Model of Preeclampsia

Davisson, Robin L.; Hoffmann, Darren S.; Butz, Genelle M.; Aldape, Gilbert; Schlager, Gunther; Merrill, David; Sethi, Sanjeev; Weiß, Robert M.; Bates, James N.

doi:10.1161/hy02t2.102904

Cited by 158 publications

(186 citation statements)

References 18 publications

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“…The disease spontaneously develops in no quadruped, although a recently described genetic mouse model by Davisson et al seems to be an exception. 11 The combination of upright posture and uteroplacental ischemia may be necessary for manifestation of the full syndrome. 12 Chronic nitric oxide synthase inhibition in rats produces a pattern of change that resembles the symptoms of preeclampsia, and the preeclamptic-like response of rats with adriamycin nephropathy and hyperinsulinemia is associated with endothelial dysfunction.…”

Section: Discussionmentioning

confidence: 99%

Agonistic Autoantibodies to the AT1 Receptor in a Transgenic Rat Model of Preeclampsia

et al. 2005

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Abstract-We used rats transgenic for the human angiotensinogen (hAogen) gene and the human renin (hRen) gene and crossed the strains to produce a model of preeclampsia in the dams. The female (nϭ9) hAogen ϫ male hRen cross had severe (telemetry-measured) hypertension and albuminuria, which developed during the last trimester of pregnancy and subsided after delivery. The converse cross (nϭ9) and control (nϭ9) SD rats did not. We demonstrated that the female hAogen ϫ male hRen cross had agonistic antibodies capable of activating the angiotensin (Ang) II AT1 receptor (AT1R-AA) and defined the epitope on the receptor's second extracellular loop. The phenomenon also occurs in humans with preeclampsia. The rats displayed renal histology reminiscent of preeclampsia, including fibrin deposition confined to the glomeruli. The complement system was activated in glomeruli and IgG deposits were present that may represent AT1R-AA. Finally, we observed an atherosis-like lesion in the spiral arteries of the placental bed, which we called placental-bed arteriolosclerosis. Our model may be relevant to preeclampsia in humans. Key Words: preeclampsia Ⅲ rats, transgenic Ⅲ antibodies Ⅲ immune systems Ⅲ renin-angiotensin system P reeclampsia, proteinuria, and severe hypertension in the latter part of pregnancy affects Ϸ3% of women in industrialized nations and a much higher percentage of women in underdeveloped countries. 1 In all countries, preeclampsia represents the major cause of maternal and fetal morbidity and mortality. Constructing a suitable animal model has been difficult. Takimoto et al described hypertension induced in pregnant mice by placental renin and maternal angiotensinogen. 2 Mice were generated transgenic for the human renin (hRen) and human angiotensinogen (hAogen) genes. The rodent and human renin-angiotensinogen systems do not interact and single transgenic animals are normotensive. Severe hypertension develops in double-transgenic offspring. The investigators observed that hypertension developed in the latter third of pregnancy in hAogen dams mated with hRen males. They showed that secreted active hRen of placental origin was capable of reacting with hAogen in the dams to produce angiotensin (Ang) II. Takimoto et al suggested that the transgenic mice might offer a unique model of "genetically induced" preeclampsia. 2 We showed that the same phenomenon exists in a rat transgenic model. 3 We used telemetric blood pressure measurements in that study to document the precise timing of the model; however, we presented no functional or histological data. 3 We have also studied preeclamptic women and found that they produce an agonistic antibody to the Ang II receptor (AT1R). 4,5 These autoantibodies (AT1-AA) activate the receptor. The activation sets into motion a chain of signaling events that could be responsible for the clinical disease. 6 We have now restudied our transgenic animal model and have observed that the rats also have these novel autoantibodies. MethodsSprague-Dawley (SD) rats harboring the human Aogen...

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Section: Discussionmentioning

confidence: 99%

Agonistic Autoantibodies to the AT1 Receptor in a Transgenic Rat Model of Preeclampsia

et al. 2005

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“…Over the past decade, various mammalian models to investigate the pathophysiology of PE have been suggested; however, their validity was hampered by the fact that in most of them, the non-pregnant control animals also developed PE-like symptoms [14][15][16][17][18][19]. Here, we introduce a new model in which activated Th1 cells are transferred into pregnant or non-pregnant recipients, which leads to PE-like symptoms exclusively in pregnant mice.…”

Section: Discussionmentioning

confidence: 99%

“…To date, some PE animal models have been proposed in the rabbit, rat and mouse [14][15][16][17][18][19]. The experimental design of such models was primarily based on mechanisms involved in the regulation of vasoconstriction/ vasodilation, i.e.…”

Section: Introductionmentioning

confidence: 99%

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Introducing a mouse model for pre‐eclampsia: adoptive transfer of activated Th1 cells leads to pre‐eclampsia‐like symptoms exclusively in pregnant mice

et al. 2004

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Pre-eclampsia (PE) is the most severe pregnancy-related disease, leading to high maternal and fetal morbidity/mortality. Immunological imbalances associated with endothelial cell dysfunction have been hypothesized as a cause for the onset and perpetuation of PE. Valid and reliable animal models are urgently required to test this hypothesis and to better understand the mechanisms underlying PE. We developed a novel PE-model by adoptively transferring activated BALB/c Th1-like splenocytes into allogeneically pregnant BALB/c female mice during late gestation; the model mimicked the symptoms of PE, i.e. increased blood pressure and glomerulonephritis accompanied by proteinuria. Interestingly, these PE-like symptoms were not detectable in non-pregnant recipients of activated Th1-like cells. Adoptive cell transfer adversely affected the outcome of pregnancy by increasing fetal rejection, with uterine immune cells showing an inflammatory profile. In conclusion, we have established a valid and reliable PE mouse model, which opens vast opportunities for therapeutic interventions.

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“…Further support for this hypothesis comes from the variety of mechanisms resulting in PE-like symptoms in mouse models. PE mouse models have been generated genetically from spontaneous hypertensive mice (5), by excessive angiotensin pathway activation (6), and by mutations affecting trophoblast cell cycle regulation (7). Interestingly, the anti-angiogenic factor, sFLT1, is present in elevated levels in the maternal circulation in most human PE pregnancies, but not all (8), and in some mouse models of PE (e.g.…”

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confidence: 99%

Translational Analysis of Mouse and Human Placental Protein and mRNA Reveals Distinct Molecular Pathologies in Human Preeclampsia

Cox

Sharma

Evangelou

et al. 2011

Molecular & Cellular Proteomics

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Preeclampsia (PE) adversely impacts ϳ5% of pregnancies. Despite extensive research, no consistent biomarkers or cures have emerged, suggesting that different molecular mechanisms may cause clinically similar disease. To address this, we undertook a proteomics study with three main goals: (1) to identify a panel of cell surface markers that distinguish the trophoblast and endothelial cells of the placenta in the mouse; (2) to translate this marker set to human via the Human Protein Atlas database; and (3) to utilize the validated human trophoblast markers to identify subgroups of human preeclampsia. To achieve these goals, plasma membrane proteins at the blood tissue interfaces were extracted from placentas using intravascular silica-bead perfusion, and then identified using shotgun proteomics. We identified 1181 plasma membrane proteins, of which 171 were enriched at the maternal blood-trophoblast interface and 192 at the fetal endothelial interface with a 70% conservation of expression in humans. Three distinct molecular subgroups of human preeclampsia were identified in existing human microarray data by using expression patterns of trophoblast-enriched proteins. Analysis of all misexpressed genes revealed divergent dysfunctions including angiogenesis (subgroup 1), MAPK signaling (subgroup 2), and hormone biosynthesis and metabolism (subgroup 3). Subgroup 2 lacked expected changes in known preeclampsia markers (sFLT1, sENG) and uniquely overexpressed GNA12. In an independent set of 40 banked placental specimens, GNA12 was overexpressed during preeclampsia when co-incident with chronic hypertension. In the current study we used a novel translational analysis to integrate mouse and human trophoblast protein expression with human microarray data. This strategy identified distinct molecular pathologies in human preeclampsia. We conclude that clinically similar

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Discovery of a Spontaneous Genetic Mouse Model of Preeclampsia

Cited by 158 publications

References 18 publications

Agonistic Autoantibodies to the AT1 Receptor in a Transgenic Rat Model of Preeclampsia

Agonistic Autoantibodies to the AT1 Receptor in a Transgenic Rat Model of Preeclampsia

Introducing a mouse model for pre‐eclampsia: adoptive transfer of activated Th1 cells leads to pre‐eclampsia‐like symptoms exclusively in pregnant mice

Translational Analysis of Mouse and Human Placental Protein and mRNA Reveals Distinct Molecular Pathologies in Human Preeclampsia

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